Direct subphthalocyanine conjugation to bombesin vs. indirect conjugation to its lipidic nanocarrier.
Fiche publication
Date publication
mai 2016
Journal
Organic & biomolecular chemistry
Auteurs
Membres identifiés du Cancéropôle Est :
Dr GONCALVES Victor, Dr DECREAU Richard
Tous les auteurs :
Bernhard Y, Gigot E, Goncalves V, Moreau M, Sok N, Richard P, Decréau RA
Lien Pubmed
Résumé
Bombesin (BBN) was covalently bound to graftable subphthalocyanine (SubPc) or to a cholesterol derivative, a component of a liposome that encapsulates non-graftable SubPc. The latter bioconjugation approach was suitable to address the stability of SubPc and was achieved by copper-free click-chemistry on the outer-face of the liposome. Liposomes were purified (FPLC) and then analyzed in size (outer diameter about 60 nm measured by DLS). In vitro binding studies allowed to determine the IC50 13.9 nM for one component of the liposome, cholesterol, conjugated to BBN. Hence, azido- (or alkynyl-) liposomes give fluorophores with no reactive functional group available on their backbone a second chance to be (indirectly) bioconjugated (with bombesin).
Référence
Org. Biomol. Chem.. 2016 May;14(19):4511-8